Literature DB >> 9447991

Mutation of Hip's carboxy-terminal region inhibits a transitional stage of progesterone receptor assembly.

V Prapapanich1, S Chen, D F Smith.   

Abstract

Steroid receptor complexes are assembled through an ordered, multistep pathway involving multiple components of the cytoplasmic chaperone machinery. Two of these components are Hsp70-binding proteins, Hip and Hop, that have some limited homology in their C-terminal regions, outside the sequences mapped for Hsp70 binding. Within this region of Hip is a DPEV sequence that occurs twice; in Hop, one DPEV sequence plus a partial second sequence occurs. In an effort to better understand Hip function as it relates to assembly of progesterone receptor complexes, the DPEV region of Hip was targeted for mutations. Each DPEV sequence was mutated to an APAV sequence, singly or in combination. The combined mutation, APAV2, was further combined with a deletion of Hip's tetratricopeptide repeat region that is required for Hsp70 binding or with a deletion of Hip's GGMP repeat. An additional mutant was prepared by truncation of Hip's DPEV-containing C terminus. By comparing interactions of various Hip forms with Hsp70, it was determined that mutation of the DPEV sequences created a dominant inhibitory form of Hip. The mutant Hip-Hsp70 complex was not prevented from interacting with progesterone receptor, but the mutant caused a dose-dependent inhibition of receptor assembly with Hsp90. The behavior of the Hip mutant is consistent with a model in which Hip and Hop are required to facilitate the transition from an early receptor complex with Hsp70 into later complexes containing Hsp90.

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Year:  1998        PMID: 9447991      PMCID: PMC108806          DOI: 10.1128/MCB.18.2.944

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  28 in total

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9.  Dynamics of heat shock protein 90-progesterone receptor binding and the disactivation loop model for steroid receptor complexes.

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  18 in total

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Review 4.  Tetratricopeptide repeat cochaperones in steroid receptor complexes.

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Review 5.  What we know about ST13, a co-factor of heat shock protein, or a tumor suppressor?

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8.  Effects of HIP in protection of HSP70 for stress-induced cardiomyocytes injury and its glucorticoid receptor pathway.

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Review 9.  Maturation of steroid receptors: an example of functional cooperation among molecular chaperones and their associated proteins.

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10.  ST13, a proliferation regulator, inhibits growth and migration of colorectal cancer cell lines.

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